Fire Retardent Chemicals Make Hand-Me-Downs Dangerous for Kids

We've known fire-retardant chemicals are dangerous for some time, but we are failing to keep them out of the hands of children.

What factors determine if you will experience healthy and cheerful aging or if it will turn into an endless chain of suffering from numerous health conditions?

Many factors shape our health, including genetics, diet, physical activity, smoking and stress. Some other factors may be as powerful but may not yet be recognized.

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I am an environmental toxicologist studying how man-made chemicals affect our health. I was always interested in understanding how our current health is shaped by chemical exposures during the embryonic and early postnatal period – life stages that are particularly sensitive to environmental stressors.

To address these questions, I focused on the analysis of long-term health effects induced by a family of chemicals used as flame retardants called polybrominated diphenyl ethers (PBDEs). The first patent for PBDE use as a flame retardant was issued in 1960, and manufacturing of commercial products containing PBDEs, such as building materials, electronics, furnishings, motor vehicles, plastics, polyurethane foams, baby pajamas and others, began in 1965. PBDEs were first detected by scientists in animal tissues in the 1980s.

Early exposures trigger lifelong changes in blood lipids

In one of my experiments, I fed mice one of the PBDEs most often found in human blood and milk – BDE-47. The female mice received itfrom day 8 of their pregnancy until the end of nursing (postpartum day 21).

We exposed mice to 0.2 milligrams of this chemical per kilogram of body weight. This caused BDE-47 concentrations in the fat of experimental animals to reach similar levels to concentrations found in humans living in big American cities. This comparison is used in toxicology to ensure that laboratory experiments use doses relevant for human exposures.

We were surprised to find that triglyceride levels were significantly altered in the offspring of exposed mothers, even though exposure to BDE-47 ceased three months earlier. Triglycerides are main constituents of body fat and cell membranes in humans and other animals.

To understand how BDE-47 changes blood triglycerides and other lipids, my laboratory conducted another experiment with mice. Lipids are insoluble molecules that are used to store energy and as structural components of cell membranes.

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We hypothesized that changes in blood lipids result from changes in liver function. It is well-known that the liver regulates composition of lipids in blood. The liver can synthesize new lipids, destroy them, secrete lipids to blood and absorb them from blood.

To test our hypothesis, we exposed female mice to BDE-47 daily during pregnancy or during the period of lactation and analyzed health outcomes in offspring when they reached one year old – roughly equivalent to 50 years in humans.

This experiment again demonstrated that short-term exposure to BDE-47 during early steps of development results in long-lasting effects on blood lipids in mice. These effects were very similar in animals that were exposed during the embryonic period or during nursing.

We observed that lower-exposure dose (0.2 mg/kg) and higher-exposure dose (1.0 mg/kg) regulated CD36 in opposite directions. Lower dose resulted in decreased CD36 and elevated blood triglycerides, while higher dose raised CD36 and decreased blood triglycerides. We think it is important to note that both tested doses were in the range of human exposures.Among key proteins involved in lipid metabolism, one was particularly high. This protein – CD36 – is responsible for pumping lipids from blood to the liver. Increased amount of CD36 in exposed animals is likely responsible for lowering lipids in blood and raising them in the liver, resulting in increased accumulation of these fats in the liver.

Do changes in CD36 pose health risks?

Our findings demonstrate that exposure to BDE-47 during early development can alter the levels of CD36 in either direction in mice and that both increase and decrease in CD36 may be deleterious.

On the other hand, decreased activity of CD36 will lead to higher lipid levels in the blood and result in atherosclerosis – a disease in which plaques of lipids build on the walls of vessels. Atherosclerosis is the primary risk factors for heart attack, which causes around 800,000 deaths annually in the U.S. alone. Thus, early life exposure to this environmental chemical may completely reprogram lifelong health trajectory.

Still at risk?

PBDEs were banned in Europe by 2008 and voluntarily withdrawn by industry in North America by 2013. It is likely that PBDEs’ production ceased all over the world, although data are missing for many regions. However these chemicals are still present in products used in U.S. households and cars. PBDEs are very stable compounds. Once released into the environment, they accumulate in sediments and in fatty tissues of wildlife and humans and stay there for many years. For example, the half-life of different PBDEs in the human body is between one and seven years. In the environment they found their way to fatty tissues of animals, many of which represent important sources of food for us.

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Although production of PBDEs has ceased in developed countries, some studies report that concentrations of PBDEs in human tissues in the U.S. continue to grow.

People born in the U.S. and Canada during the last 15 to 20 years were exposed during their early life to environmental concentrations of PBDE, comparable to those that reprogrammed lipid metabolism in our experiments with mice. Thus, we believe that about 20 percent of the North American population may be at risk of conditions associated with altered lipid concentrations in blood and liver.

It is not yet clear if effects of these other chemicals are as long-lasting as effects of PBDE. It is also not yet clear if effects of chemical exposures observed in mice are the same in humans. Mice are the most widely used animal model for testing the toxicity of pharmaceuticals and industrial chemicals, and animal toxicology studies generally are applicable to humans, although responses of laboratory animals and humans to chemicals may differ in type and severity.